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zadetkov: 19
1.
  • Oligomerization‐driven MLKL... Oligomerization‐driven MLKL ubiquitylation antagonizes necroptosis
    Liu, Zikou; Dagley, Laura F; Shield‐Artin, Kristy ... EMBO journal, 01 December 2021, Letnik: 40, Številka: 23
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    Mixed lineage kinase domain‐like (MLKL) is the executioner in the caspase‐independent form of programmed cell death called necroptosis. Receptor‐interacting serine/threonine protein kinase 3 (RIPK3) ...
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2.
  • Conformational interconvers... Conformational interconversion of MLKL and disengagement from RIPK3 precede cell death by necroptosis
    Garnish, Sarah E; Meng, Yanxiang; Koide, Akiko ... Nature communications, 04/2021, Letnik: 12, Številka: 1
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    Phosphorylation of the MLKL pseudokinase by the RIPK3 kinase leads to MLKL oligomerization, translocation to, and permeabilization of, the plasma membrane to induce necroptotic cell death. The ...
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3.
  • Human RIPK3 maintains MLKL ... Human RIPK3 maintains MLKL in an inactive conformation prior to cell death by necroptosis
    Meng, Yanxiang; Davies, Katherine A; Fitzgibbon, Cheree ... Nature communications, 11/2021, Letnik: 12, Številka: 1
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    The ancestral origins of the lytic cell death mode, necroptosis, lie in host defense. However, the dysregulation of necroptosis in inflammatory diseases has led to widespread interest in targeting ...
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4.
  • Identification of MLKL memb... Identification of MLKL membrane translocation as a checkpoint in necroptotic cell death using Monobodies
    Petrie, Emma J.; Birkinshaw, Richard W.; Koide, Akiko ... Proceedings of the National Academy of Sciences - PNAS, 04/2020, Letnik: 117, Številka: 15
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    The necroptosis cell death pathway has been implicated in host defense and in the pathology of inflammatory diseases. While phosphorylation of the necroptotic effector pseudokinase Mixed Lineage ...
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5.
  • Distinct pseudokinase domai... Distinct pseudokinase domain conformations underlie divergent activation mechanisms among vertebrate MLKL orthologues
    Davies, Katherine A; Fitzgibbon, Cheree; Young, Samuel N ... Nature communications, 06/2020, Letnik: 11, Številka: 1
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    The MLKL pseudokinase is the terminal effector in the necroptosis cell death pathway. Phosphorylation by its upstream regulator, RIPK3, triggers MLKL's conversion from a dormant cytoplasmic protein ...
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6.
  • Rare catastrophes and evolu... Rare catastrophes and evolutionary legacies: human germline gene variants in MLKL and the necroptosis signalling pathway
    Garnish, Sarah E; Hildebrand, Joanne M Biochemical Society transactions, 02/2022, Letnik: 50, Številka: 1
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    Programmed cell death has long been characterised as a key player in the development of human disease. Necroptosis is a lytic form of programmed cell death that is universally mediated by the ...
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7.
  • MLKL trafficking and accumu... MLKL trafficking and accumulation at the plasma membrane control the kinetics and threshold for necroptosis
    Samson, Andre L; Zhang, Ying; Geoghegan, Niall D ... Nature communications, 06/2020, Letnik: 11, Številka: 1
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    Mixed lineage kinase domain-like (MLKL) is the terminal protein in the pro-inflammatory necroptotic cell death program. RIPK3-mediated phosphorylation is thought to initiate MLKL oligomerization, ...
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8.
  • Phosphorylation-dependent p... Phosphorylation-dependent pseudokinase domain dimerization drives full-length MLKL oligomerization
    Meng, Yanxiang; Garnish, Sarah E; Davies, Katherine A ... Nature communications, 10/2023, Letnik: 14, Številka: 1
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    Abstract The necroptosis pathway is a lytic, pro-inflammatory mode of cell death that is widely implicated in human disease, including renal, pulmonary, gut and skin inflammatory pathologies. The ...
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10.
  • Membrane permeabilization i... Membrane permeabilization is mediated by distinct epitopes in mouse and human orthologs of the necroptosis effector, MLKL
    Sethi, Ashish; Horne, Christopher R; Fitzgibbon, Cheree ... Cell death and differentiation, 09/2022, Letnik: 29, Številka: 9
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    Necroptosis is a lytic programmed cell death pathway with origins in innate immunity that is frequently dysregulated in inflammatory diseases. The terminal effector of the pathway, MLKL, is licensed ...
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Dostopno za: UL
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zadetkov: 19

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